© j. straus 2002 casrip 2002 high technology protection summit seattle, july 20, 2002 ethical...
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© J. Straus 2002
CASRIP 2002 High Technology Protection SummitSeattle, July 20, 2002
Ethical Issues in Patent Law Biotechnology and Research Ethics
- A European Perspective –
Joseph Straus, Munich
• Ethical Considerations and Patenting in Europe
• Ordre Public & Morality vs. Patents – Complex Relationship
• Agreement on Trade Related Aspects of IPR (TRIPS) (1994) the
Controlling Rule
• EU-Directive on the Legal Protection of Biotechnological
Inventions 98/44/EC (1998) & Implementing Regulations to the
EPC (1999)
• Patenting of Human Stem Cells as Most Recent Example
• Outlook
© J. Straus 2002
Ethical Considerations and Patenting in Europe
Exclusionary Provisions in EPC & National Laws
• Methods for treatment of the human or animal body by surgery or therapy and diagnostic methods practised on the human or animal body – not however products, i.e. substances or compositions, for use in any of these methods.*
[Art. 52 (4) EPC]
• Inventions the publication or exploitation of which would be contrary to „ordre public“** or morality*** - simple prohibitions of exploitation not sufficient
[Art. 53 (a) EPC]
* Thus methods employed and products used in and resulting from somatic gene therapy and somatic cell therapy patentable.
** To be construed as referring to the most fundamental rules of the relevant legal order.
*** To be construed as embracing only high-ranking and generally accepted ethical principles.
© J. Straus 2002
Ordre Public & Morality vs. Patents
Complex Relationship
• Ordre public and morality depending on:
– Actual state of science and technology (e.g. feasibility, safety, etc.)
– Social acceptance of technology at hand
– Can be changed and adapted accordingly at will
• Patents
– Exclusive rights granted for 20 years
– No license to use the patented invention
– Once an invention becomes state of the art – no patent protection available
– Traditionally – no specific exclusionary provisions, but general clauses only – ordre public and morality – allowing flexible response – specific exclusions – allow no flexible response – if removed – no retroactive effects
© J. Straus 2002
Controlling TRIPS Rules
• Patents must be available for any inventions in all fields of
technology, without discrimination as to the place of invention or
to the place of production – if the usual patentability criteria are
met.
[Art. 27 (1)]
• WTO Members may exclude from patentability inventions if their
commercial exploitation would violate ordre public or morality
(protection of human, animal or plant life or health or
environment) mere prohibition of exploitation not sufficient – in
any case, commercialisation of such inventions may not be
allowed!!![Art. 27 (2)]
© J. Straus 2002
Controlling TRIPS Rules
• WTO Members may further exclude from patentability inventions
of diagnostic, therapeutic and surgical methods for treatment of
humans and animals, ....
[Art. 27 (3 (a)]
• These principles of TRIPS are explicitly acknowledged in the EU-
Directive 98/44/EC
[Recital 12, Art. 1 (2)]
continued
© J. Straus 2002
EU-Directive on the Legal Protection of Biotechnological Inventions
98/44/EC of 1998 and Ethics
• The Commission‘s European Group on Ethics in Science and
Technology evaluates all ethical aspects of biotechnology.
[Art. 7]
• The Group may be consulted only when biotechnology is to be
evaluated at the level of basic ethical principles, including such
patent law issues.
[Art. 7 Recitals 19, 44]
© J. Straus 2002
EU-Directive on the Legal Protection of Biotechnological Inventions 98/44/EC of 1998
Excluded from Patentability
• The human body at various stages of its formation and development – principle of non-commercialisation of the human body Art. 5 (1)]
• Inventions, the commercial exploitation of which would be contrary to ordre public or morality – mere prohibitions not sufficient - as such considered, in particular:
– Processes for cloning human beings– Processes for modifying the germ line genetic identity of
human beings– Uses of human embryos for industrial or commercial purposes– Processes for modifying the genetic identity of animals likely
to cause them suffering without any substantial medical benefit to man or animal and the resulting animals
[Art. 6 (1) (2)]
© J. Straus 2002
EU-Directive on the Legal Protection of Biotechnological Inventions 98/44/EC of 1998
Excluded from Patentability
• Generally accepted rule: Excluded only if this being the only
possible (claimed) use
• Ordre public and morality correspond in particular to ethical or
moral principles recognized in a Member State
[Recital 39]
• Consensus exists that the cloning of human beings offends
against ordre public and morality[Recital 40]
continued
© J. Straus 2002
EU-Directive on the Legal Protection of Biotechnological Inventions 98/44/EC of 1998
Excluded from Patentability
• Process for cloning human beings – any process, including
techniques of embryo splitting, designed to create a human being
with the same nuclear genetic information as another living or
deceased human being
[Recital 41]
• Inventions for therapeutic or diagnostic purposes applied to the h-
embryo and useful to it – not affected by exclusions
[Recital 42]
continued
© J. Straus 2002
EU-Directive on the Legal Protection of
Biotechnological Inventions 98/44/EC of 1998
However patentable
• Elements of the human body, including sequences or partial
sequences of a gene – if isolated or otherwise technically
produced even if structure identical to the natural one
[Art. 5 (2)]
• Prior free and informed consent of the donor, in accordance with
national laws required
[Recital 26]
continued
© J. Straus 2002
European Court of Justice (ECJ) on EU-Directive 98/44/EC
Case C-377/98 of October 9, 2001
• Confirmed the legality of the Directive
• Observed that the „ordre public or morality“ rule in principle
allows patent offices and courts of the Member States a wide
scope for manoeuvre in applying this exclusion
• Observed that that scope of manoeuvre necessary to take account
of the particular difficulties to which the use of certain patents
may give rise in the social and cultural context of each Member
State, a context which the national legislative, administrative or
court authorities are better placed to undertake than are the
Community authorities
© J. Straus 2002
European Court of Justice (ECJ) on EU-Directive 98/44/EC
Case C-377/98 of October 9, 2001
• The scope left to Member States not discretionary, its limits:
– Prohibition of exploitation not sufficient
– Four specific – mandatory – exclusions
• Fundamental Rights to human dignity and integrity observed and guaranteed [Art. 5 (1) (2), Art. 6]
• Observed that the prior free and informed consent of the donor and recipient outside the scope of the Directive and to be dealt by other laws
• Clarified that the Directive does not preclude legal limitations and prohibitions applying to research into patentable products or the exploitation of patented products – i.e., research exemption
continued
© J. Straus 2002
Opinion No. 15 of the EU Group on Ethics in Science and New
Technologies (EGE) of November 2000
• EGE recommended as regards human stem cell research and its
uses:
– To set up a strict public control by centralized authorities, on
human embryo research where it is allowed;
– To take measures to prevent commercialisation of human
embryos or cadaveric foetal tissue;
– To ensure the respect of ethical principles through the control
of public authorities, concerning import of human stem cells.
© J. Straus 2002
Opinion No. 16 of the EU Group on Ethics in Science and New Technologies (EGE) of May 2002
• EGE observed that it would be contrary to public (and especially
patients) interests, if patenting of stem cells or stem cell lines
would be forbidden
• Isolated stem cells which have not been modified do not, as
product, fulfil the legal requirements for patentability. Moreover,
such cells are so close to the human body, to the foetus or to the
embryo they have been isolated from, that their patenting may be
considered as a form of commercialisation of the human body
• Unmodified stem cell lines can hardly be considered as a
patentable product. They do not have a specific use but a very
large range of potential undescribed uses
© J. Straus 2002
Opinion No. 16 of the EU Group on Ethics in Science and New
Technologies (EGE) of May 2002
• Stem cell lines which have been modified by in-vitro treatments, or genetically modified so that they have acquired characteristics for specific industrial application, fulfil the legal requirements for patentability
• Processes involving human stem cells, whatever their source, patentable
• Applicants for a patent involving human stem cells should declare which is the source of the stem cells
• Patenting of inventions allowing the transformation of unmodified stem cells from human embryonic origin into genetically modified stem cell lines or specific differentiated stem cell lines for specific therapeutic or other uses – ethically acceptable
continued
© J. Straus 2002
Opinion No. 16 of the EU Group on Ethics in Science and New Technologies (EGE) of May 2002
• Donors should be informed of the possibility of patenting and
they are entitled to refuse such use
• Apart from justified compensation, donors should not get a
reward which could infringe the principle of non-
commercialisation of the human body
• In addition to the research exemption, it is essential to secure that
patents on stem cell lines are not too broad
• EGE-considers that there may be also a need to make ethical
evaluations in the course of the examination of patent
applications involving specific ethical dimensions
continued
© J. Straus 2002
UK Human Fertilization and Embryology Act (HFE Act 1990) and
German Embryo Protection Act (EPA 1990) – Two Extremes
• HFE Act administered by Human Fertilisation and Embryology Authority (HFEA)– prohibits cloning involving "replacing the nucleus of a cell of
an embryo with a nucleus taken from a cell of any person"– permits licensed research on human embryos of up to 14 days
of development
The following constitutes criminal offence:carry out any treatment using h-embryos outside the body- use donated gametes- store any oocytes, sperm or embryos, or- undertake any research on h-embryo without a license from
the HFEA
Somatic Cell Nuclear Transfer (SCNT) involving nuclear substitution into an unfertilized egg - not an embryo - not covered
© J. Straus 2002
UK Human Fertilization and Embryology Act (HFE Act 1990) and
German Embryo Protection Act (EPA 1990) – Two Extremes
Guidelines (DOH, MRC) exist for using pluripotent stem cell lines (imported into or developed in the UK)
HFEA may license such research only if necessary or desirable for either of the following purposes:- promoting advances in the treatment of infertility- increasing knowledge about the causes of congenital disease- increasing knowledge about the causes of miscarriage- developing more effective contraception techniques- developing methods for detecting the presence of gene or
chromosome abnormalities in embryo before implantation- other purposes as may be specified in regulations by the
Secretary of State, e.g. - developing methods of therapy for mitochondrial diseases- developing methods of therapy for diseased or damaged
tissues or organs
continued
© J. Straus 2002
UK Human Fertilization and Embryology Act (HFE Act 1990) and
German Embryo Protection Act (EPA 1990) – Two Extremes
• German EPA – Basic Principles
– The prohibitions aimed at safeguarding human dignity and protection of life from its inception
– Embryo any fertilized egg (oocyte) capable of development, from the fusion of nuclei, i.e. the fusion of chromosomes of an oocyte and a sperm cell leading to the formation of a novel individual genome
– As embryo considered also all totipotent cells removed from an embryo, which have the innate capacity to divide and develop into an individual being provided that suitable further requirements are met
continued
© J. Straus 2002
UK Human Fertilization and Embryology Act (HFE Act 1990) and
German Embryo Protection Act (EPA 1990) – Two Extremes
• Cloning a criminal offence: artificial generation of a human embryo with the same genetic information as another embryo, foetus, or human being, whether living or dead
• Interference with the development of an embryo permitted solely if it serves the welfare of the embryo
• Prohibited:– the preparation of ES cells from blastocysts – nuclear transfer into enucleated oocytes because a totipotent
cell is generated
• Allowed:– the removal of primordial germ cells from dead foetuses for
scientific, therapeutical, or diagnostic purposes
[Sec. 6,8; DFG interpretation]
continued
© J. Straus 2002
Patent DE 197 56 864 C1 of April 29, 1999
Inventor: Dr. O. Brüstle
Neural precursors, method of production and use for therapy of
neural defects
Claims:
1. Isolated, purified precursor cells with neuronal or glial characteristics from embryonic stem cells1)2) containing at most about 15% of primitive embryonic and non-neural cells, obtainable through the following steps:
a) culturing of ES-cells to embryoid bodies
b) ....
5. Cells according to one of the Claims 1-4, whereby the embryonic stem cells from oocytes are obtained after a nuclear transplantation
© J. Straus 2002
Patent DE 197 56 864 C1 of April 29, 1999
Inventor: Dr. O. Brüstle
6. Cells according to one of the Claims 1-4, whereby the embryonic stem cells are obtained from embryonic germ cells
7. Cells according to one of the Claims 1-6, whereby the cells are mamalian cells
8. Cells according Claim 7, whereby the cells are from the group encompassing mice, rat, hamster, pig, beef, primates or human being were isolated
.....
12.Method for the production of purified precursor cells ...., encompassing the following steps:
a) culturing of ES cells to embryoid bodies,
....
continued
© J. Straus 2002
Patent DE 197 56 864 C1 of April 29, 1999Inventor: Dr. O. Brüstle
Definitions
• ES-cells can be obtained, e.g. from very early embryos in the
blastocyst stage. These are totipotent cells, which can be kept in
undifferentiated stage through many passages, and which
possess the ability to differentiate in all tissues and cell types
[Specification p. 4 l. 33-36]
• The term toti-, pluri-, multi- and bipotent cells stands for precursor
cells which differenciate in all (totipotent), many different (pluri- or
multipotent) or two (bipotent) mature cell types.
[Specification p. 4 l. 53-55]
© J. Straus 2002
Patent DE 197 56 864 C1 of April 29, 1999Inventor: Dr. O. Brüstle
Interpretation by the German Patent Office
• Production of totipotent cells by nuclear transfer - not covered by Sec. 8 EPA, because neither a fertilisation takes place nor is a totipotent cell removed from an embryo
• The point in time of accomplishment of reprogramming of nucleus corresponding to fusion of nuclei cannot be established - whether this has taken place can only be demonstrated by later development into a mature individual
• This does not apply here because purified precursor cells with neural and glial properties are produced and no viable individuals
© J. Straus 2002
Patent DE 197 56 864 C1 of April 29, 1999Inventor: Dr. O. Brüstle
Interpretation by the German Patent Office
• The "totipotent" cells of the invention are actually not totipotent because they were removed from the inner cell mass (Embryoblast) which without foreign blastocyst cannot develop into a mature individual
• Embryonal germ cells of the invention are cells of Embryoblasts, which can differentiate into all tissues and cell types, but cannot form Trophoblasts and have, thus, lost the capability to develop into an individual
• Inventor is not obliged to strictly observe legal definitions. Decisive is the meaning which an expert can derive from the description and whether the expert can successfully repeat the invention
© J. Straus 2002
Perspectives of Ordre Public and Morality in Future European
Practice in Biotech Area
• Direct linking of patentability with specific prohibitions of exploitation based on ethical considerations – doubtful approach
• Harmonized interpretation of Article 6 EU-Directive 98/44/EC and the respective national patent law provisions needed - otherwise the Directive cannot achieve its goals
• This includes the interpretation of such terms as "cloning", "human being" and "embryo" according to a "European Standard"
• Key role of the European Court of Justice in future setting of standards
© J. Straus 2002
Perspectives of Ordre Public and Morality in Future European Practice in Biotech Area
• Since a patent not a license to use - national regulatory provisions will continue to control the use - exploitation of the technology - but should also be harmonized
• To avoid, or at least, reduce negative economic impact resulting
from possible future changes of regulatory provisions (deletion of
prohibitory provisions), patent law exclusions should be
interpreted narrowly
• Stem cell technology should be used as an example why the
legislator should refrain from specific exclusions from
patentability
continued